4.8 Article

Time-Resolved Small RNA Sequencing Unravels the Molecular Principles of MicroRNA Homeostasis

Journal

MOLECULAR CELL
Volume 75, Issue 4, Pages 756-+

Publisher

CELL PRESS
DOI: 10.1016/j.molcel.2019.06.018

Keywords

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Funding

  1. Austrian Academy of Sciences
  2. Austrian Science Fund FWF [Y-733-B22 START, W127-B09, F4322]
  3. European Research Council [ERC-StG-338252 miRLIFE, ERC-PoC-825710 SLAMseq]
  4. Austrian Science Fund (FWF) [Y733] Funding Source: Austrian Science Fund (FWF)

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Argonaute-bound microRNAs silence mRNA expression in a dynamic and regulated manner to control organismal development, physiology, and disease. We employed metabolic small RNA sequencing for a comprehensive view on intracellular microRNA kinetics in Drosophila. Based on absolute rate of biogenesis and decay, microRNAs rank among the fastest produced and longest-lived cellular transcripts, disposing up to 10(5) copies per cell at steady-state. Mature microRNAs are produced within minutes, revealing tight intracellular coupling of biogenesis that is selectively disrupted by pre-miRNA-uridylation. Control over Argonaute protein homeostasis generates a kinetic bottleneck that cooperates with non-coding RNA surveillance to ensure faithful microRNA loading. Finally, regulated small RNA decay enables the selective rapid turnover of Ago1-bound microRNAs, but not of Ago2-bound small interfering RNAs (siRNAs), reflecting key differences in the robustness of small RNA silencing pathways. Time-resolved small RNA sequencing opens new experimental avenues to deconvolute the timescales, molecular features, and regulation of small RNA silencing pathways in living cells.

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